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Colorectal Hyperplasia and Dysplasia Due to Human Carcinoembryonic Antigen (CEA) Family Member Expression in Transgenic Mice

机译:大肠增生和异型增生归因于人类癌胚抗原(CEA)家族成员在转基因小鼠中的表达。

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摘要

CEA and CEACAM6 are immunoglobulin family intercellular adhesion molecules that are up-regulated without structural mutations in approximately 70% of human cancers. Results in in vitro systems showing tumorigenic effects for these molecules suggest that this correlation could indicate an instrumental role in tumorigenesis. To test whether this applies in vivo, transgenic mice harboring 187 kb of the human genome containing four CEA family member genes including the CEA and CEACAM6 genes were created and their copy numbers increased by mating until colonocyte expression levels reached levels seen in human colorectal carcinomas. The colonocyte surface level of integrin α5 and the activation of AKT increased progressively with the expression levels of CEA/CEACAM6. Colonic crypts showed a progressive increase in colonocyte proliferation, an increase in crypt fission, and a strong inhibition of both differentiation and anoikis/apoptosis. All transgenic mice showed massively enlarged colons comprising a continuous mosaic of severe hyperplasia, dysplasia and serrated adenomatous morphology. These results suggest that up-regulated non-mutated adhesion molecules could have a significant instrumental role in human cancer.
机译:CEA和CEACAM6是免疫球蛋白家族的细胞间粘附分子,在大约70%的人类癌症中被上调而没有结构突变。体外系统显示出这些分子的致瘤作用的结果表明,这种相关性可能表明在致瘤作用中的重要作用。为了测试这是否适用于体内,创建了包含187 kb的人类基因组的转基因小鼠,该基因组包含四个CEA家族成员基因,包括CEA和CEACAM6基因,并通过交配直至结肠细胞表达水平达到人大肠癌中的水平来增加其拷贝数。随着CEA / CEACAM6的表达水平,整联蛋白α5的结肠细胞表面水平和AKT的活化逐渐增加。结肠隐窝显示结肠细胞增殖逐渐增加,隐窝裂变增加,并且强烈抑制分化和失神经/凋亡。所有转基因小鼠均显示出大量肿大的结肠,其中包括严重增生,异型增生和锯齿状腺瘤形态的连续镶嵌。这些结果表明,上调的非突变粘附分子可能在人类癌症中具有重要的工具作用。

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